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Would Kraepelin reconsider the distinction between schizophrenia and bipolar disorder if he had access to recent molecular genetics evidence?

Published online by Cambridge University Press:  04 December 2013

Ole A. Andreassen*
Affiliation:
NORMENT, K.G. Jebsen Centre for Psychosis Research, Institute of Clinical Medicine, University of Oslo and Division of Mental Health and Addiction, Oslo University Hospital, Oslo, Norway E-mail: [email protected]
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Abstract

Type
Editorial
Copyright
Copyright © Scandinavian College of Neuropsychopharmacology 2013 

Emil Kraepelin divided psychotic disorders into two distinct categories, dementia praecox and manic-depressive illness (Reference Beer1). This dichotomous classification has been maintained in the ICD and recently updated in DSM diagnostic systems, but there is clearly overlapping phenotypes between the diagnoses of schizophrenia and bipolar disorder as well as schizoaffective disorders (Reference Simonsen, Sundet and Vaskinn2). Further, several authors have argued for the continuum model, with prototypic bipolar disorder in one end and prototypic schizophrenia in the other (Reference Craddock and Owen3). These models are all based on descriptive symptomatology and not on underlying mechanisms (Reference Kendler4). Epidemiological studies have shown that schizophrenia and bipolar disorder run in families (Reference Lichtenstein, Yip and Bjork5), and provided support for shared genetic risk factors. Twin studies have estimated heritability rates to be ∼80% for both disorders (Reference Purcell, Wray and Stone6,Reference Smoller and Finn7). With the recent progress in technology in the genetics field, it has been proposed that molecular genetics may help inform the nosology of severe mental disorders.

The microarray genotyping technology has provided a boost to psychiatric genetics. This has enabled genotyping of unprecedented large samples (Reference Purcell, Wray and Stone6,Reference Stefansson, Ophoff and Steinberg8), and facilitated by the international Psychiatric Genomics Consortium (PGC; https://pgc.unc.edu/index.php), a series of recent large genome-wide association studies (GWAS) has been conducted. These have identified several new common risk variants [single nucleotide polymorphisms (SNPs)] associated with psychotic disorders (Reference Ripke, Sanders and Kendler9,Reference Sklar, Ripke and Scott10). A recent PGC cross-disorder mega-analysis (n = 33 332 cases, n = 27 888 controls) investigating schizophrenia, bipolar disorder, major depressive disorder, autism spectrum disorders and attention-deficit hyperactivity disorder identified common risk variants (SNPs) for all five disorders (11). Among these disorders, the strongest overlap in genetic risk was observed between schizophrenia and bipolar disorder. In addition to common variants (SNPs), rare structural variants called copy number variants (CNVs) have been found associated with schizophrenia (Reference Stefansson, Rujescu and Cichon12). Interestingly, CNVs seem not to be associated with bipolar disorder to the same degree (Reference Bergen, O'Dushlaine and Ripke13). Thus, there is evidence for shared as well as disease-specific genetic risk for schizophrenia and bipolar disorder. This supports the hypothesis of partial genetic overlap between the two disorders, which was the rationale for the study by Gu et al. (Reference Gu, Tan and Su14) In this issue of the journal. Gu et al. performed a meta-analysis of eight studies with schizophrenia (n = 2953 cases, n = 3153 controls) and six studies of bipolar disorder (n = 923 cases, n = 928 controls), focusing on the 1354C/T genetic polymorphism of 5-hydroxytryptamine receptor 2A. In their samples with both Caucasian and Asian ethnicity, they did not find any association with this gene marker for neither schizophrenia nor bipolar disorder. This negative finding is in line with the concept of overlapping genetic risk factors in these disorders.

However, the single SNP approach is not able to capture much of the heritability of these disorders. Recently, new evidence for a polygenic architecture of bipolar disorder and schizophrenia was presented. The first evidence for a polygenic overlap in psychotic disorders came from a combined GWAS (Reference Purcell, Wray and Stone6), where the cumulative risk from the entire genome is extracted from one GWAS dataset to predict risk in an independent sample (Reference Purcell, Wray and Stone6). As schizophrenia and bipolar disorder share common genetic risk, we have applied new statistical methods to leverage the pleiotropy between the two disorders to improve gene discovery, that is, use information on risk variants identified in one disorder to improve detection of risk variants in the other (Reference Andreassen, Thompson and Schork15). Based on these Bayesian methods, it is also possible to estimate the total number of SNPs associated with these disorders. These analyses suggest that there are ∼12 000 SNPs associated with both schizophrenia and bipolar disorders. Further, these new statistical methods for analysing GWAS results of polygenic complex disorders can also be used to identify potential common biological pathways, as illustrated with schizophrenia and cardiovascular disease risk factors (Reference Andreassen, Djurovic and Thompson16).

The advance in our understanding of the underlying genetic architecture of bipolar disorder and schizophrenia may have a large potential for generating new knowledge about the pathophysiology of these major neuropsychiatric disorders – which may eventually also lead to better diagnostic systems as well as new drug development.

References

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